Defects of glycosyltransferase activities in human fibroblasts of Pk and p blood group phenotypes.

AUTOR(ES)

Kijimoto-Ochiai, S

RESUMO

We demonstrate that human fibroblasts of the rare Pk phenotype lack globoside, which was identified as the blood group P antigen, and that p cells possess neither globoside nor trihexosyl ceramide, which was identified as Pk antigen. Our investigations indicate also that these glycosphingolipid patterns are most likely caused by inherited preferential biosynthetic pathways in the abnormal phenotypes rather than by excess catabolism of the antigens. Evidence is presented that the fibroblasts of Pk phenotype lack beta-N-acetylgalactosaminyltransferase (globoside synthetase; UDP-N-acetylgalactosamine:trihexosylceramide beta-N-acetylgalactosaminyltransferase; EC 2.4.1.79) activity, and those of p are deficient in alpha-galactosyltransferase (trihexosylceramide synthetase; UDP galactose:lactosylceramide alpha-galactosyltransferase) and possibly also in globoside synthetase. The diminished globoside synthetase activity in p cells, however, is not caused by the defect in the gene coding for this enzyme. It appears, rather, to be caused by a failure in gene expression because one-third of Pk X p hybrids became able to express P antigenicity with a time lag of 3-4 days after cell fusion [Fellous, M., Gerbal, A., Nobillot, G. & Weils, J. (1977) Vox Sang. 32, 262-268].

Documentos Relacionados

• Direct Measurement of the pK Values of an Alkaline Bohr Group in Human Hemoglobin
• Haptoglobin phenotypes.
• Zellweger syndrome and associated phenotypes.
• Chromosome 1p terminal deletion: report of new findings and confirmation of two characteristic phenotypes.
• Deletions in the 5' region of dystrophin and resulting phenotypes.